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胸苷酸合成酶互补蛋白的底物和辅因子复合结构的功能分析

Functional analysis of substrate and cofactor complex structures of a thymidylate synthase-complementing protein.

作者信息

Mathews Irimpan I, Deacon Ashley M, Canaves Jaume M, McMullan Daniel, Lesley Scott A, Agarwalla Sanjay, Kuhn Peter

机构信息

Stanford Synchrotron Radiation Laboratory, Stanford University, 2575 Sand Hill Road, SSRL MS 69, Menlo Park, CA 94025, USA.

出版信息

Structure. 2003 Jun;11(6):677-90. doi: 10.1016/s0969-2126(03)00097-2.

Abstract

Like thymidylate synthase (TS) in eukaryotes, the thymidylate synthase-complementing proteins (TSCPs) are mandatory for cell survival of many prokaryotes in the absence of external sources of thymidylate. Details of the mechanism of this novel family of enzymes are unknown. Here, we report the structural and functional analysis of a TSCP from Thermotoga maritima and its complexes with substrate, analogs, and cofactor. The structures presented here provide a basis for rationalizing the TSCP catalysis and reveal the possibility of the design of an inhibitor. We have identified a new helix-loop-strand FAD binding motif characteristic of the enzymes in the TSCP family. The presence of a hydrophobic core with residues conserved among the TSCP family suggests a common overall fold.

摘要

与真核生物中的胸苷酸合成酶(TS)一样,胸苷酸合成酶互补蛋白(TSCPs)对于许多原核生物在缺乏胸苷酸外源供应时的细胞存活至关重要。这个新型酶家族的作用机制细节尚不清楚。在此,我们报告了来自嗜热栖热菌的一种TSCP及其与底物、类似物和辅因子复合物的结构和功能分析。这里展示的结构为解释TSCP催化作用提供了基础,并揭示了设计抑制剂的可能性。我们鉴定出了TSCP家族中该酶特有的一种新的螺旋-环-链FAD结合基序。TSCP家族中保守残基形成的疏水核心的存在表明其具有共同的整体折叠结构。

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